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Everything you always wanted to know about TB… but were afraid to inhale? Kevin Schwartzman MD, MPH Respiratory Division, MUHC [email protected] McGill Internal Medicine Resident Core Teaching March 29, 2012
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Everything you always wanted to know about TB…but were afraid to inhale? Kevin Schwartzman MD, MPH Respiratory Division, MUHC [email protected].

Dec 17, 2015

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Page 1: Everything you always wanted to know about TB…but were afraid to inhale? Kevin Schwartzman MD, MPH Respiratory Division, MUHC kevin.schwartzman@mcgill.ca.

Everything you always wanted to know about TB…but were afraid to inhale?

Kevin Schwartzman MD, MPHRespiratory Division, MUHC

[email protected]

McGill Internal Medicine Resident Core TeachingMarch 29, 2012

Page 2: Everything you always wanted to know about TB…but were afraid to inhale? Kevin Schwartzman MD, MPH Respiratory Division, MUHC kevin.schwartzman@mcgill.ca.

Question

What is special about March 24?

http://www.youtube.com/watch?v=6tynGqZV1A0

www.theunion.org www.stoptb.org

Page 3: Everything you always wanted to know about TB…but were afraid to inhale? Kevin Schwartzman MD, MPH Respiratory Division, MUHC kevin.schwartzman@mcgill.ca.

Learner Objectives--1

To describe basic concepts in tuberculosis epidemiology

To recognize the spectrum of clinical and radiographic manifestations of active TB, in different patient populations

To describe the essential pathophysiology of latent and active TB

To identify and understand the rationale for evidence-based diagnostic strategies for active TB

Page 4: Everything you always wanted to know about TB…but were afraid to inhale? Kevin Schwartzman MD, MPH Respiratory Division, MUHC kevin.schwartzman@mcgill.ca.

Learner Objectives--2

To describe standard treatment for active TB

To identify indications, contraindications, and potential complications of this treatment

To identify key concepts in TB control, within and outside the hospital

Page 5: Everything you always wanted to know about TB…but were afraid to inhale? Kevin Schwartzman MD, MPH Respiratory Division, MUHC kevin.schwartzman@mcgill.ca.

Overview

Case presentations Epidemiology Pathophysiology Active TB:

Diagnosis Treatment, including special considerations Infection control

Key concepts in TB control

Page 6: Everything you always wanted to know about TB…but were afraid to inhale? Kevin Schwartzman MD, MPH Respiratory Division, MUHC kevin.schwartzman@mcgill.ca.

Jad Davenport, “Mural outside tuberculosis clinic, Dhaka”World Lung Foundation (http://worldlungfoundation.org)

Page 7: Everything you always wanted to know about TB…but were afraid to inhale? Kevin Schwartzman MD, MPH Respiratory Division, MUHC kevin.schwartzman@mcgill.ca.

Jad Davenport. “TB flourishes in crowded Dhaka shantytowns”World Lung Foundation (http://worldlungfoundation.org)

Page 8: Everything you always wanted to know about TB…but were afraid to inhale? Kevin Schwartzman MD, MPH Respiratory Division, MUHC kevin.schwartzman@mcgill.ca.

Pierre Virot, “A TB patient is examined by the doctor, Ghana”World Lung Foundation (http://worldlungfoundation.org)

Page 9: Everything you always wanted to know about TB…but were afraid to inhale? Kevin Schwartzman MD, MPH Respiratory Division, MUHC kevin.schwartzman@mcgill.ca.

www.nytimes.comOn May 24, 2007, Andrew Speaker, a 31 year-old lawyer from Atlanta, landed at Trudeau Airport on a flight from Prague, with a diagnosis of extensively drug-resistant (XDR) tuberculosis. He drove a rented car across the US border, and was apprehended. He had smear-negative TB, later determined not to be XDR.

Page 10: Everything you always wanted to know about TB…but were afraid to inhale? Kevin Schwartzman MD, MPH Respiratory Division, MUHC kevin.schwartzman@mcgill.ca.

Case 1

35 y.o. Inuit female Referred to MGH after trauma Smoker, no other past history No respiratory or constitutional symptoms Previously exposed to brother with active

TB Apparently did not receive treatment for latent

infection

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Next steps?

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Case 1

Underwent bronchoscopy BAL cytology negative BAL smear-negative for AFB

Discharged to the North with instructions for follow-up CXRs and clinical follow-up/other tests depending on results BAL ultimately culture-negative

Apparently lost to follow-up until she developed left arm and shoulder pain months later

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Case 1

What would you recommend now?

Page 17: Everything you always wanted to know about TB…but were afraid to inhale? Kevin Schwartzman MD, MPH Respiratory Division, MUHC kevin.schwartzman@mcgill.ca.

Case 1

Bronchoscopy: some mucosal abnormalities seen on left side

BAL AFB smear negative BUT necrotizing granulomatous

inflammation and AFB seen on biopsy specimens

Patient is staying at Northern Module What would you recommend now?

Page 18: Everything you always wanted to know about TB…but were afraid to inhale? Kevin Schwartzman MD, MPH Respiratory Division, MUHC kevin.schwartzman@mcgill.ca.

Case 2

32 y.o. male refugee claimant from Congo, arrived in Canada < 1 week previously

Admitted to medical ward because of extensive herpes zoster in left V1 distribution, with probable bacterial superinfection

Wife known HIV-positive, no respiratory issues Patient found to be HIV-positive with CD4 70 Complains of minor hemoptysis

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Case 2

What investigations (if any) would you now arrange?

Would you isolate this patient? What treatment (if any) would you

recommend?

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Case 3

40 year-old female, Quebec-born, referred for persistent cough of 6 months’ duration

Smoker; also noticed ~10 lbs weight loss No travel history, no known HIV risks

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Ms CL

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Case 3

What would be your differential diagnosis? What would be your next steps?

Page 24: Everything you always wanted to know about TB…but were afraid to inhale? Kevin Schwartzman MD, MPH Respiratory Division, MUHC kevin.schwartzman@mcgill.ca.

“I thought TB had disappeared”

2010: WHO estimated 8.8 million new cases, vs. 8.3 million cases in 2000 and 6 million cases in 1990

40% in India and China, 24% in Africa Overall global incidence 128 per 100,000

annually, down from peak 142 in 2004 1.1 million deaths in HIV-negative individuals,

350,000 deaths in HIV-positive individuals 1/3 of world population believed to have latent

TB infection

http://www.who.int/tb/publications/global_report/en/index.html

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Major Determinants

Basic elements of TB control e.g. diagnosis, consistent and appropriate treatment

Health system infrastructure e.g. national control programs, public vs. private providers etc.

General socioeconomic and health status, tobacco, alcohol, diabetes

HIV Drug resistance Obviously all these are interrelated

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Bates et al, Arch Int Med 2007

Smoking and TB

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Diabetes and TB

Jeon and Murray, PLoS Medicine 2008

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HIV

Strongest known risk factor for TB disease Increases risk of progression/reactivation

of latent TB infection by 100-fold or more To date, impact on global epidemiology

most evident in sub-Saharan Africa, but concern re unknown magnitude of HIV-TB coinfection notably in India

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Drug Resistance

In 2010, the estimated number of prevalent cases of multi-drug resistant TB was 650,000 (of 12 million prevalent cases of active TB overall)

Estimated that 3.4% of new cases and 20% of retreatment cases were MDR-TB

Defined as resistance to isoniazid AND rifampin, with or without resistance to other antibiotics

A marker of treatment program quality Poor prognosis, treatment complexity and

expense

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Page 34: Everything you always wanted to know about TB…but were afraid to inhale? Kevin Schwartzman MD, MPH Respiratory Division, MUHC kevin.schwartzman@mcgill.ca.

WHO, Anti-Tuberculosis Drug Resistance in the World, 2008

Page 35: Everything you always wanted to know about TB…but were afraid to inhale? Kevin Schwartzman MD, MPH Respiratory Division, MUHC kevin.schwartzman@mcgill.ca.

WHO, Anti-Tuberculosis Drug Resistance in the World, 2008

Page 36: Everything you always wanted to know about TB…but were afraid to inhale? Kevin Schwartzman MD, MPH Respiratory Division, MUHC kevin.schwartzman@mcgill.ca.

TB in Canada

Ellis et al, Public Health Agency of Canada

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Montreal

123 reported active TB cases in 2007; maximum was 209 in 1994

Corresponding decrease in incidence from 11.6 to 6.4 per 100,000

Consistently ~80% of cases involve foreign-born persons

DSP Montréal-Centre, Bureau de surveillance épidémiologique

http://www.santepub-mtl.qc.ca/Mi/surveillance/mado/archives/90-2005/incidence90-2007.pdf

Page 43: Everything you always wanted to know about TB…but were afraid to inhale? Kevin Schwartzman MD, MPH Respiratory Division, MUHC kevin.schwartzman@mcgill.ca.

Active Tuberculosis

Airborne Droplets

Inhalation by Others

Latent Infection

Case Finding (Passive or Active)

Effective Drug Treatment

Patient Behaviour (e.g. Cover Mouth)

Respiratory Isolation

Ventilation and Air Filtration

Ultraviolet Light

Progression or Reactivation

Antiretroviral Therapy for HIV

BCG Vaccination

Diagnosis and Treatment of Latent TB

Pathophysiology

Page 44: Everything you always wanted to know about TB…but were afraid to inhale? Kevin Schwartzman MD, MPH Respiratory Division, MUHC kevin.schwartzman@mcgill.ca.

Long and Schwartzman, Transmission and Pathogenesis of TB, Chapter 3, Canadian Tuberculosis Standards 2007

Page 45: Everything you always wanted to know about TB…but were afraid to inhale? Kevin Schwartzman MD, MPH Respiratory Division, MUHC kevin.schwartzman@mcgill.ca.

Clinical Manifestations

Pulmonary disease: 2/3 of cases in Canada Pleural TB and thoracic nodal disease ~ 10% Most common extrapulmonary site is peripheral lymph

nodes (~12%) Patients often asymptomatic when they have

less extensive disease (e.g. immigration screening)

Most frequent symptom: cough, usually for weeks to months—in symptomatic patients, virtually always present (even if not the symptom that precipitated the visit)

Page 46: Everything you always wanted to know about TB…but were afraid to inhale? Kevin Schwartzman MD, MPH Respiratory Division, MUHC kevin.schwartzman@mcgill.ca.

Clinical Manifestations

Other frequent symptoms: sputum, fever, malaise, loss of weight/appetite, night sweats, hemoptysis

Symptoms generally not very specific, hence the importance of the clinical and epidemiologic context

Timing of cough often used to estimate period of contagion

Physical exam generally not helpful; may show cachexia, fever, sometimes adenopathy

Page 47: Everything you always wanted to know about TB…but were afraid to inhale? Kevin Schwartzman MD, MPH Respiratory Division, MUHC kevin.schwartzman@mcgill.ca.

Questions to Ask

Place of birth, year of immigration (risk highest in years immediately after arrival)

Known history of TB disease, latent TB, exposure

Recent travel Visitors from abroad HIV issues Other past medical history

Page 48: Everything you always wanted to know about TB…but were afraid to inhale? Kevin Schwartzman MD, MPH Respiratory Division, MUHC kevin.schwartzman@mcgill.ca.

Chest Radiograph

The key first step in investigation A normal chest X-ray usually excludes the

diagnosis of pulmonary TB, except in some HIV-infected persons

Reactivation disease: usually upper zone airspace disease (infiltrate; “fluffy” appearance), may have cavities Involvement of other areas of lung, or contralateral

lung, suggests bronchogenic spread, and a higher bacterial load/potential for contagion

Beware of judging active vs. inactive TB on a CXR

Page 49: Everything you always wanted to know about TB…but were afraid to inhale? Kevin Schwartzman MD, MPH Respiratory Division, MUHC kevin.schwartzman@mcgill.ca.

Gary Hampton, “Paula Fujiwara of the IUATLD talks to the mother of a TB patient…” World Lung Foundation (http://worldlungfoundation.org)

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Chest X-Ray

Primary disease (usually children, or persons with advanced HIV infection): lower zone disease, often dense consolidation, with or without cavitation May mimic bacterial pneumonia May be associated with intrathoracic

adenopathy

Miliary disease (rare)

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Ms GL

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Diagnosis of Active TB

For pulmonary disease, diagnosis hinges on growth of mycobacteria from respiratory secretions, i.e. sputum (spontaneous or induced), and/or bronchoalveolar lavage

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Diagnosis

Culture of a single induced sputum has similar sensitivity to BAL culture for the diagnosis of pulmonary TB

3 induced sputa may have better sensitivity than BAL

Page 59: Everything you always wanted to know about TB…but were afraid to inhale? Kevin Schwartzman MD, MPH Respiratory Division, MUHC kevin.schwartzman@mcgill.ca.

Diagnosis

For other sites, biopsy (showing necrotizing granulomas, and ideally acid-fast bacteria) and/or culture according to the site Very low yield of fluid smear and culture for

serosal disease (pleural, pericardial, peritoneal)

Biopsies needed, with histology and culture

Page 60: Everything you always wanted to know about TB…but were afraid to inhale? Kevin Schwartzman MD, MPH Respiratory Division, MUHC kevin.schwartzman@mcgill.ca.

Diagnosis

For pulmonary TB, typically 50-60% smear-positive, though this will vary with clinical context Lower with HIV, or persons diagnosed

because of screening (e.g. immigration, contacts)

Higher with more advanced symptoms, more extensive radiographic abnormalities

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Standard Nucleic Acid Amplification (PCR)

Limited use in diagnosis of smear-negative pulmonary TB, or extrapulmonary disease Sensitivity typically reported to be ~60% for

smear-negative pulmonary disease Lower for extrapulmonary disease A negative result cannot be used to exclude the

diagnosis Occasionally ordered under very specific

circumstances e.g. contact investigation that will start sooner if PCR positive

Page 62: Everything you always wanted to know about TB…but were afraid to inhale? Kevin Schwartzman MD, MPH Respiratory Division, MUHC kevin.schwartzman@mcgill.ca.

Menzies and Khan, Diagnosis of Tuberculosis Infection and Disease, Chapter 4, Canadian Tuberculosis Standards, 2007

Page 63: Everything you always wanted to know about TB…but were afraid to inhale? Kevin Schwartzman MD, MPH Respiratory Division, MUHC kevin.schwartzman@mcgill.ca.

Nucleic Acid Amplification

Now used as standard method to confirm that an isolate is M. tuberculosis AFB smear-positive specimens Cultures growing mycobacteria

Final confirmation is performed at the provincial reference laboratory

Page 64: Everything you always wanted to know about TB…but were afraid to inhale? Kevin Schwartzman MD, MPH Respiratory Division, MUHC kevin.schwartzman@mcgill.ca.

What’s new?

http://www.who.int/tb/features_archive/xpert_use_web/en/

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Page 66: Everything you always wanted to know about TB…but were afraid to inhale? Kevin Schwartzman MD, MPH Respiratory Division, MUHC kevin.schwartzman@mcgill.ca.

Reporting

Once identified in the laboratory, reporting of active TB to public health authorities is mandatory by law “Double reporting” by laboratory and treating

physician Treating physician must report cases treated

on the basis of clinical diagnosis alone

Treatment of contagious tuberculosis is also required by law, and can be imposed

Page 67: Everything you always wanted to know about TB…but were afraid to inhale? Kevin Schwartzman MD, MPH Respiratory Division, MUHC kevin.schwartzman@mcgill.ca.

Tuberculin Skin Testing and Interferon-Gamma Release Assays

Are NOT appropriate diagnostic tests for active TB

A positive test may indicate TB infection, but cannot distinguish active from latent TB Pre-test probability of latent TB infection may

be 50% or higher, depending on the patient’s origin

Page 68: Everything you always wanted to know about TB…but were afraid to inhale? Kevin Schwartzman MD, MPH Respiratory Division, MUHC kevin.schwartzman@mcgill.ca.

Tuberculin Skin Testing and Interferon-Gamma Release Assays

Well-known false negative rate of ≥ 10% in active TB A negative TST or IGRA does not exclude the

diagnosis

False negatives also seen with HIV, other immune suppression e.g. in rheumatologic disease, transplant Anergy screens poorly reliable in this context

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Initiating Treatment

Empiric treatment for active TB may sometimes be started without culture confirmation

This depends on the perceived likelihood of active TB, the potential consequences of waiting for confirmation, and the potential risks of treatment

Page 70: Everything you always wanted to know about TB…but were afraid to inhale? Kevin Schwartzman MD, MPH Respiratory Division, MUHC kevin.schwartzman@mcgill.ca.

Initiating Treatment

Treatment for latent TB should NEVER be started if active disease is a possibility If cultures have been sent, await results before

treating for latent TB (if appropriate)

However, it IS acceptable to initiate treatment for active TB, then modify if cultures are negative 4-month modified regimen for “culture-negative” TB

Also beware of treating pneumonia with a fluoroquinolone, if TB is a possibility

Page 71: Everything you always wanted to know about TB…but were afraid to inhale? Kevin Schwartzman MD, MPH Respiratory Division, MUHC kevin.schwartzman@mcgill.ca.

Treatment

Intensive phase: first 2 months Daily isoniazid, rifampin, pyrazinamide, and

ethambutol

Continuation phase: usually 4 additional months Daily or intermittent isoniazid and rifampin

• If intermittent, must be directly observed PZA stopped after 2 month intensive phase Ethambutol discontinued once drug susceptibility

confirmed

Page 72: Everything you always wanted to know about TB…but were afraid to inhale? Kevin Schwartzman MD, MPH Respiratory Division, MUHC kevin.schwartzman@mcgill.ca.

Treatment

Isoniazid: 5 mg/kg, to 300 mg max plus pyridoxine 25 mg daily

Rifampin: 10 mg/kg, to 600 mg max

Ethambutol: 15 mg/kg, to 1600 mg max

Pyrazinamide: 20 mg/kg, to 2000 mg max

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Toxicity

Liver: pyrazinamide > isoniazid > rifampin Asymptomatic transaminase rises are much more

common than overt hepatitis

Skin rashes: same Neuropathy: isoniazid Hematologic: rifampin Hypersensitivity, flu-like: rifampin Optic neuropathy: ethambutol [Orange discolouration: rifampin]

Page 74: Everything you always wanted to know about TB…but were afraid to inhale? Kevin Schwartzman MD, MPH Respiratory Division, MUHC kevin.schwartzman@mcgill.ca.

From Yee et al, Am J Respir Crit Care Med 2003. Bars show isoniazid, rifampin and PZA in that order, except for visual disturbance with ethambutol.

Standard definition of hepatitis was used, i.e. transaminases ≥ 3 x upper limit of normal with symptoms, or ≥ 5 x upper limit without symptoms

Page 75: Everything you always wanted to know about TB…but were afraid to inhale? Kevin Schwartzman MD, MPH Respiratory Division, MUHC kevin.schwartzman@mcgill.ca.

Special Considerations

Drug interactions Rifampin: potent P450 inducer

• Warfarin, antiretrovirals, cyclosporin, tacrolimus, oral contraceptives, anti-seizure medications, etc.

Isoniazid: increases phenytoin levels

Hepatic disease: close supervision May consider avoiding PZA, substituting

moxifloxacin

Active TB patients are usually seen at least monthly after discharge

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Special Considerations

Renal dysfunction Dose adjustment for ethambutol Pyrazinamide is dialyzed Both given 3 times weekly for dialysis patients

Pregnancy INH, rifampin, ethambutol safe Safety of pyrazinamide undocumented, so

usually avoided No quinolones

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Special Considerations

HIV Timing of antiretroviral therapy in patients with

new diagnosis of HIV concomitant with TB (Earlier appears better)

Immune reconstitution Drug-drug interactions Drug absorption Length of treatment

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Length of Treatment

Usually 6 months Extended to 9 months if culture-positive at 2

months Also extended for bone or joint disease, CNS

disease (12 months)

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Other Considerations

Adjunctive corticosteroids TB meningitis Pericardial TB

Therapeutic drug monitoring Clinical response slower than expected Concern about absorption or interactions

Direct observation Drug resistance

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Infection Control

Most important: institution of appropriate isolation, diagnostics and treatment

Use of negative pressure room Use of N95 masks

Patients can use surgical masks when outside their rooms

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Infection Control Smear-positive patients usually hospitalized

until repeatedly smear-negative Occasional exceptions for patients who live

alone and will remain at home

Smear-negative patients may be treated as outpatients, depending on the home situation and prospects for adherence Admission of patients with young children Admission of patients from congregate settings

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Long and Schwartzman, Transmission and Pathogenesis of TB, Chapter 3, Canadian Tuberculosis Standards 2007

Page 83: Everything you always wanted to know about TB…but were afraid to inhale? Kevin Schwartzman MD, MPH Respiratory Division, MUHC kevin.schwartzman@mcgill.ca.

Contact Investigation

An important element of TB control in industrialized countries

“Concentric circle” approach for patients with pulmonary disease, beginning with household contacts

More extensive investigation for patients with smear-positive or laryngeal disease Also extended if there is evidence of significant

transmission, e.g. secondary active cases or excessive latent infection in contacts

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Contact Investigation

One of the most cost-effective TB prevention strategies

Contacts diagnosed with latent TB infection are a high priority for treatment Active TB MUST be excluded

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Key Concepts in TB Control

Priority is diagnosis and treatment of the most infectious patients WHO “DOTS” strategy focuses on diagnosis

using sputum smear microscopy Appropriate and complete drug treatment,

most often with direct supervision Monitoring and documentation of treatment

outcomes Major limitations include HIV, drug

resistance

Page 86: Everything you always wanted to know about TB…but were afraid to inhale? Kevin Schwartzman MD, MPH Respiratory Division, MUHC kevin.schwartzman@mcgill.ca.

Key Concepts in TB Control

Adjuncts to improve diagnostic yield Enhanced microscopy GeneXpert MTB/RIF® Availability of mycobacterial cultures in some settings

Linkage of TB and HIV control activities Rethinking empiric TB retreatment strategies to

deal with resistance Better MDR coverage Increasing the availability of drug susceptibility testing

Page 87: Everything you always wanted to know about TB…but were afraid to inhale? Kevin Schwartzman MD, MPH Respiratory Division, MUHC kevin.schwartzman@mcgill.ca.

Key Concepts in TB Control

In middle- and high-income countries, contact investigation with treatment of latent infection among contacts at risk

In the US and Canada, targeted testing and treatment for latent TB infection

Immigration-related screening activities Detection and treatment of active TB at time of

immigration Detection and potential treatment of “high-risk”

inactive TB

Page 88: Everything you always wanted to know about TB…but were afraid to inhale? Kevin Schwartzman MD, MPH Respiratory Division, MUHC kevin.schwartzman@mcgill.ca.

Summary

TB remains a major global health problem Although incidence has decreased in Canada

(and Montreal), we will continue to see it Foreign-born, Aboriginals, homeless,

immunosuppressed

Essential to keep the diagnosis of TB in mind, and pursue it using the right tools, in the appropriate clinical, radiographic, and epidemiologic context

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Summary

Active TB Importance of microbiologic diagnosis;

biopsy/histology for extrapulmonary disease Standard treatment regimens Suitable respiratory isolation

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THANK YOU! WHO/TBP/Jan van den Hombergh, Ethiopian girls in Assosa Mooi (World Lung Foundation)